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转录组-蛋白质组关联研究揭示了复杂性状的顺式和反式调控机制。

Transcriptome-wide association study of the plasma proteome reveals cis and trans regulatory mechanisms underlying complex traits.

机构信息

Program in Bioinformatics, Loyola University Chicago, Chicago, IL 60660, USA.

Broad Institute of MIT and Harvard, Cambridge, MA 02142, USA.

出版信息

Am J Hum Genet. 2024 Mar 7;111(3):445-455. doi: 10.1016/j.ajhg.2024.01.006. Epub 2024 Feb 5.

Abstract

Regulation of transcription and translation are mechanisms through which genetic variants affect complex traits. Expression quantitative trait locus (eQTL) studies have been more successful at identifying cis-eQTL (within 1 Mb of the transcription start site) than trans-eQTL. Here, we tested the cis component of gene expression for association with observed plasma protein levels to identify cis- and trans-acting genes that regulate protein levels. We used transcriptome prediction models from 49 Genotype-Tissue Expression (GTEx) Project tissues to predict the cis component of gene expression and tested the predicted expression of every gene in every tissue for association with the observed abundance of 3,622 plasma proteins measured in 3,301 individuals from the INTERVAL study. We tested significant results for replication in 971 individuals from the Trans-omics for Precision Medicine (TOPMed) Multi-Ethnic Study of Atherosclerosis (MESA). We found 1,168 and 1,210 cis- and trans-acting associations that replicated in TOPMed (FDR < 0.05) with a median expected true positive rate (π) across tissues of 0.806 and 0.390, respectively. The target proteins of trans-acting genes were enriched for transcription factor binding sites and autoimmune diseases in the GWAS catalog. Furthermore, we found a higher correlation between predicted expression and protein levels of the same underlying gene (R = 0.17) than observed expression (R = 0.10, p = 7.50 × 10). This indicates the cis-acting genetically regulated (heritable) component of gene expression is more consistent across tissues than total observed expression (genetics + environment) and is useful in uncovering the function of SNPs associated with complex traits.

摘要

转录和翻译的调控是遗传变异影响复杂性状的机制。与顺式调控(转录起始位点附近 1Mb 内)相比,表达数量性状基因座(eQTL)研究在鉴定顺式 eQTL 方面更为成功。在这里,我们测试了基因表达的顺式成分与观察到的血浆蛋白水平之间的关联,以鉴定调节蛋白水平的顺式和反式作用基因。我们使用来自 49 个基因型-组织表达(GTEx)项目组织的转录组预测模型来预测基因表达的顺式成分,并测试了每个组织中每个基因的预测表达与 INTERVAL 研究中 3301 个人观察到的 3622 种血浆蛋白丰度之间的关联。我们在来自 Trans-omics for Precision Medicine (TOPMed) 多民族动脉粥样硬化研究(MESA)的 971 个人中测试了显著结果的复制。我们在 TOPMed 中发现了 1168 个和 1210 个顺式和反式作用关联,其复制的 FDR<0.05,中位数预期真实阳性率(π)在组织中分别为 0.806 和 0.390。反式作用基因的靶蛋白在 GWAS 目录中富集了转录因子结合位点和自身免疫疾病。此外,我们发现同一潜在基因的预测表达和蛋白质水平之间的相关性更高(R=0.17),而观察到的表达(R=0.10,p=7.50×10)则较低。这表明基因表达的顺式作用遗传调节(可遗传)成分比总观察到的表达(遗传+环境)在组织中更一致,并且有助于揭示与复杂性状相关的 SNP 的功能。

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